Litcius/Paper detail

Androgen-Independent Prostate Cancer Is Sensitive to CDC42-PAK7 Kinase Inhibition

Hyun Ho Han, Cheol Keun Park, Young Deuk Choi, Nam Hoon Cho, Jong Soo Lee, Kang Su Cho

2022Biomedicines16 citationsDOIOpen Access PDF

Abstract

Prostate cancer is a common form of cancer in men, and androgen-deprivation therapy (ADT) is often used as a first-line treatment. However, some patients develop resistance to ADT, and their disease is called castration-resistant prostate cancer (CRPC). Identifying potential therapeutic targets for this aggressive subtype of prostate cancer is crucial. In this study, we show that statins can selectively inhibit the growth of these CRPC tumors that have lost their androgen receptor (AR) and have overexpressed the RNA-binding protein QKI. We found that the repression of microRNA-200 by QKI overexpression promotes the rise of AR-low mesenchymal-like CRPC cells. Using in silico drug/gene perturbation combined screening, we discovered that QKI-overexpressing cancer cells are selectively vulnerable to CDC42-PAK7 inhibition by statins. We also confirmed that PAK7 overexpression is present in prostate cancer that coexists with hyperlipidemia. Our results demonstrate a previously unseen mechanism of action for statins in these QKI-expressing AR-lost CRPCs. This may explain the clinical benefits of the drug and support the development of a biology-driven drug-repurposing clinical trial. This is an important finding that could help improve treatment options for patients with this aggressive form of prostate cancer.

Topics & Concepts

Prostate cancerAndrogen deprivation therapyCancer researchAndrogen receptorFLNACDC42CancerMedicineCancer cellInternal medicineBiologyKinaseCellCell biologyGeneticsFilaminCytoskeletonCancer, Lipids, and MetabolismProstate Cancer Treatment and ResearchRNA Research and Splicing